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Doxycycline ameliorates the dystrophic phenotype of skeletal and cardiac muscles in mdx mice

机译:强力霉素可改善mdx小鼠骨骼肌和心肌的营养不良表型

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Introduction: We examined whether doxycycline, an antibiotic member of the tetracycline family, improves the histopathology and muscle function in mdx mice, the experimental model of DMD. Methods: Doxycycline was administered for 36 days (starting on postnatal day 0) and for 9 months (starting at 8 months of age) in drinking water. Histopathological, biochemical (creatine kinase), and functional (forelimb muscle grip strength) parameters were evaluated in limb, diaphragm, and cardiac muscle. Results: Doxycycline significantly minimized the dystrophic phenotype of skeletal and cardiac muscles and improved forelimb muscle strength. The drug protected muscle fibers against myonecrosis and reduced inflammation. Furthermore, it slowed the progression of myocardial fibrosis. Conclusions: This study provides evidence that doxycycline may be a potential therapeutic agent for DMD.
机译:简介:我们检查了四环素家族的抗生素成员多西环素是否能改善mdx小鼠(DMD的实验模型)的组织病理学和肌肉功能。方法:多西环素在饮用水中给药36天(从出生后第0天开始),为期9个月(从出生后8个月开始)。在肢体,diaphragm肌和心肌中评估了组织病理学,生化(肌酸激酶)和功能(前臂抓地力)参数。结果:强力霉素可最大程度地减少骨骼肌和心肌的营养不良表型,并改善前肢肌肉的力量。该药物可保护肌纤维免受坏死并减少炎症。此外,它减慢了心肌纤维化的进程。结论:这项研究提供了证据证明强力霉素可能是DMD的潜在治疗剂。

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